Publikation: Pre-existing clusters of the adaptor Lat do not participate in early T cell signaling events
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2011
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Williamson, David J.
Owen, Dylan M.
Magenau, Astrid
Wehrmann, Matthias
Gooding, J. Justin
Gaus, Katharina
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Nature Immunology. 2011, 12(7), pp. 655-663. ISSN 1529-2908. eISSN 1529-2916. Available under: doi: 10.1038/ni.2049
Zusammenfassung
Engaged T cell antigen receptors (TCRs) initiate signaling through the adaptor protein Lat. In quiescent T cells, Lat is segregated into clusters on the cell surface, which raises the question of how TCR triggering initiates signaling. Using super-resolution fluorescence microscopy, we found that pre-existing Lat domains were neither phosphorylated nor laterally transported to TCR activation sites, which suggested that these clusters do not participate in TCR signaling. Instead, TCR activation resulted in the recruitment and phosphorylation of Lat from subsynaptic vesicles. Studies of Lat mutants confirmed that recruitment preceded and was essential for phosphorylation and that both processes were independent of surface clustering of Lat. Our data suggest that TCR ligation preconditions the membrane for vesicle recruitment and bulk activation of the Lat signaling network.
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570 Biowissenschaften, Biologie
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WILLIAMSON, David J., Dylan M. OWEN, Jérémie ROSSY, Astrid MAGENAU, Matthias WEHRMANN, J. Justin GOODING, Katharina GAUS, 2011. Pre-existing clusters of the adaptor Lat do not participate in early T cell signaling events. In: Nature Immunology. 2011, 12(7), pp. 655-663. ISSN 1529-2908. eISSN 1529-2916. Available under: doi: 10.1038/ni.2049BibTex
@article{Williamson2011-06-05Preex-43445,
year={2011},
doi={10.1038/ni.2049},
title={Pre-existing clusters of the adaptor Lat do not participate in early T cell signaling events},
number={7},
volume={12},
issn={1529-2908},
journal={Nature Immunology},
pages={655--663},
author={Williamson, David J. and Owen, Dylan M. and Rossy, Jérémie and Magenau, Astrid and Wehrmann, Matthias and Gooding, J. Justin and Gaus, Katharina}
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<dcterms:abstract xml:lang="eng">Engaged T cell antigen receptors (TCRs) initiate signaling through the adaptor protein Lat. In quiescent T cells, Lat is segregated into clusters on the cell surface, which raises the question of how TCR triggering initiates signaling. Using super-resolution fluorescence microscopy, we found that pre-existing Lat domains were neither phosphorylated nor laterally transported to TCR activation sites, which suggested that these clusters do not participate in TCR signaling. Instead, TCR activation resulted in the recruitment and phosphorylation of Lat from subsynaptic vesicles. Studies of Lat mutants confirmed that recruitment preceded and was essential for phosphorylation and that both processes were independent of surface clustering of Lat. Our data suggest that TCR ligation preconditions the membrane for vesicle recruitment and bulk activation of the Lat signaling network.</dcterms:abstract>
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